New Cytotoxic α-Aminoacylamide and bis-1,5-Disubstituted Tetrazole Adducts From Amino-Diterpene Molecules by Ugi Reaction

IF 3.2 4区医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Chemical Biology & Drug Design Pub Date : 2024-09-22 DOI:10.1111/cbdd.14632

Anna Smirnova, Elena Tretyakova, Oxana Kazakova

引用次数: 0

Abstract

In search for new molecules of diterpene origin with promising anticancer activity, two amino-derivatives (methyl maleopimarate aminoimide and methyl 1β,13-epoxydihydroquinopimarate C4-hydrazone) were involved in the 4-component Ugi reaction (Ugi-4CR) and pseudo-7-component azido-Ugi condensation (azido-Ugi-7CR) to afford a series of adducts holding α-aminoacylamide and bis-1,5-disubstituted tetrazole substituents. The NCI-60 cancer cell panel screening revealed diterpene-type Ugi adducts 2, 5, and 6 with strong antiproliferative potency with GI₅₀ in range of 1.2–15.4 μM. The high positive correlations with standard anticancer drugs suggest microtubules or progesterone and androgen receptors as possible targets of the synthesized compounds.

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通过乌基反应从氨基二萜分子中分离出具有细胞毒性的α-氨基乙酰胺和双-1,5-二取代四氮唑加合物

为了寻找具有抗癌活性的二萜新分子，两种氨基衍生物（马来酰亚胺酸甲酯氨基亚胺和 1β、13-epoxydihydroquinopimarate C4-hydrazone）参与了 4 组分 Ugi 反应（Ugi-4CR）和假 7 组分叠氮-Ugi 缩合反应（叠氮-Ugi-7CR），生成了一系列含有 α-氨基乙酰胺和双-1,5-二取代四氮唑取代基的加合物。通过对 NCI-60 癌细胞面板的筛选，发现二萜型 Ugi 加合物 2、5 和 6 具有很强的抗增殖效力，GI50 在 1.2-15.4 μM 之间。与标准抗癌药物的高度正相关性表明，微管或孕酮和雄激素受体可能是合成化合物的靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Chemical Biology & Drug Design 医学-生化与分子生物学

CiteScore

5.10

自引率

3.30%

发文量

164

审稿时长

4.4 months

期刊介绍： Chemical Biology & Drug Design is a peer-reviewed scientific journal that is dedicated to the advancement of innovative science, technology and medicine with a focus on the multidisciplinary fields of chemical biology and drug design. It is the aim of Chemical Biology & Drug Design to capture significant research and drug discovery that highlights new concepts, insight and new findings within the scope of chemical biology and drug design.